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超分辨率和相关双采样在冷冻电子显微镜中的应用。

Application of super-resolution and correlative double sampling in cryo-electron microscopy.

机构信息

Diamond Light Source, Harwell Science and Innovation Campus, Didcot, OX11 0DE, UK.

RCaH, Harwell Science and Innovation Campus, Didcot, OX11 0DE, UK.

出版信息

Faraday Discuss. 2022 Nov 8;240(0):261-276. doi: 10.1039/d2fd00049k.

Abstract

Developments in cryo-EM have allowed atomic or near-atomic resolution structure determination to become routine in single particle analysis (SPA). However, near-atomic resolution structures determined using cryo-electron tomography and sub-tomogram averaging (cryo-ET STA) are much less routine. In this paper, we show that collecting cryo-ET STA data using the same conditions as SPA, with both correlated double sampling (CDS) and the super-resolution mode, allowed apoferritin to be reconstructed out to the physical Nyquist frequency of the images. Even with just two tilt series, STA yields an apoferritin map at 2.9 Å resolution. These results highlight the exciting potential of cryo-ET STA in the future of protein structure determination. While processing SPA data recorded in super-resolution mode may yield structures surpassing the physical Nyquist limit, processing cryo-ET STA data in the super-resolution mode gave no additional resolution benefit. We further show that collecting SPA data in the super-resolution mode, with CDS activated, reduces the estimated -factor, leading to a reduction in the number of particles required to reach a target resolution without compromising the data size on disk and the area imaged in SerialEM. However, collecting SPA data in CDS does reduce throughput, given that a similar resolution structure, with a slightly larger -factor, is achievable with optimised parameters for speed in EPU (without CDS).

摘要

冷冻电镜技术的发展使得单颗粒分析(SPA)中的原子分辨率或近原子分辨率结构测定成为常规操作。然而,利用冷冻电子断层扫描和子断层平均(cryo-ET STA)确定的近原子分辨率结构则不那么常见。在本文中,我们展示了使用与 SPA 相同的条件收集 cryo-ET STA 数据,同时使用相关双采样(CDS)和超分辨率模式,可以将脱铁蛋白重构到图像的物理奈奎斯特频率。即使只有两个倾斜系列,STA 也能得到 2.9Å分辨率的脱铁蛋白图谱。这些结果突出了 cryo-ET STA 在未来蛋白质结构测定中的令人兴奋的潜力。虽然处理超分辨率模式下记录的 SPA 数据可能会产生超过物理奈奎斯特极限的结构,但在超分辨率模式下处理 cryo-ET STA 数据并不能获得额外的分辨率优势。我们进一步表明,在超分辨率模式下收集带有 CDS 的 SPA 数据可以降低估计的因子,从而减少达到目标分辨率所需的粒子数量,而不会影响磁盘上的数据大小和 SerialEM 中的成像区域。然而,在 CDS 中收集 SPA 数据确实会降低吞吐量,因为使用优化的参数可以以更快的速度获得具有稍大因子的类似分辨率结构(没有 CDS)。

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